Association of μ‐opioid receptor gene polymorphism (A118G) with variations in morphine consumption for analgesia after total knee arthroplasty

Chou, Wei‐Yang; Yang, Lan-Yan; Lu, Hsin-Chun; Ko, Jui‐Hung; Wang, Chi-Hui; Lin, Shang-Hung; Lee, T.‐H.; Concejero, Allan M.; Hsu, Chien Jen

doi:10.1111/j.1399-6576.2006.01058.x

Cited by 283 publications

(201 citation statements)

References 18 publications

Supporting

Mentioning

175

Contrasting

Unclassified

Order By: Relevance

“…morphine via patient-controlled analgesia [10,11,14,23]. In these various settings, patients with at least one 304G allele exhibited a trend towards increased systemic morphine requirements, findings which are in the opposite direction to our results with intrathecal fentanyl.…”

Section: Discussioncontrasting

confidence: 55%

Genetic variability of the μ-opioid receptor influences intrathecal fentanyl analgesia requirements in laboring women ☆

Landau

Kern

Columb

et al. 2008

Pain

137

View full text Add to dashboard Cite

Labor initiates one of the most intensely painful episodes in a woman's life. Opioids are used to provide analgesia with substantial interindividual variability in efficacy. μ-Opioid receptor (μOR, OPRM1) genetic variants may explain differences in response to opioid analgesia. We hypothesized that OPRM1 304A/G polymorphism influences the median effective dose (ED 50 ) of intrathecal fentanyl via combined spinal-epidural for labor analgesia. Nulliparous women were prospectively recruited around 35 weeks gestation (n = 224), and genotyped for 304A/G polymorphism. Those requesting neuraxial labor analgesia were enrolled in one of the two double-blinded trials: up-down sequential allocation (SA, n = 50) and a separate confirmatory random-dose allocation trial (RA, n = 97). Effective analgesia from intrathecal fentanyl was defined by ⩾ 60 min analgesia with verbal rating score ≤1 (scale 0-10) and was compared between μOR 304A homozygotes (Group A) and women carrying at least one 304G allele (Group G). OPRM1 304G allele frequency f(−) was 0.18. Using SA, intrathecal fentanyl ED 50 was 26.8 μg (95% CI 22.7-30.9) in Group A and 17.7 μg (95% CI 13.4-21.9) in Group G (p < 0.001; 304A homozygosity increased the ED 50 1.5-fold). RA confirmed that 304A homozygosity significantly increases intrathecal fentanyl ED 50 (27.4 μg in Group A and 12.8 μg in Group G [p < 0.002; 2.1-fold]). We demonstrate for the first time that the μOR 304G variant significantly reduces intrathecal fentanyl ED 50 for labor analgesia, suggesting women with the G variant may be more responsive to opioids and require less analgesic drugs. These Conflict of interestNone of the authors presents any commercial association or other issues that might pose a conflict of interest. Financial disclosures

show abstract

Section: Discussioncontrasting

confidence: 55%

Genetic variability of the μ-opioid receptor influences intrathecal fentanyl analgesia requirements in laboring women ☆

Landau

Kern

Columb

et al. 2008

Pain

137

View full text Add to dashboard Cite

show abstract

“…Few studies have investigated the effect of the Il8A>G polymorphism on post-operative pain or its interaction with other opioids. Two studies were conducted on an Asian population undergoing scheduled gynaecological and orthopaedic surgery: they received POP therapy with morphine by means of PCA (Patient-Controlled-Analgesia) over 48 h: female G 118G homozygotes needed more morphine (33± IOmg) in the first postoperative day than A l18G heterozygotes (29±8mg) or wild-type (27± 1Omg) (19,20). More recently, a study conducted on 138 Japanese patients, undergoing major open abdominal surgery, confirmed that G118G homozygous Assessed for eligibility (n=801 consecutive scheduled surgery'patients)…”

Section: Discussionmentioning

confidence: 99%

Micro Opioid Receptor A118G Polymorphism and Post-Operative Pain: Opioids' Effects on Heterozigous Patients

Capraris

Cinnella

Marolla

et al. 2011

Int J Immunopathol Pharmacol

View full text Add to dashboard Cite

The Single-Nucleotide-Polymorphism (SNP) 118A>G in the 1l-1 Opioid Receptor gene (OPRM1) is associated with a decrease in the analgesic effects of opioids. The aim of this study is to assess whether 118A>G polymorphism could influence the analgesic response to opioid-based postoperative pain (POP) therapy. The study consisted of two parts: section a, observational, included 199 subjects undergoing scheduled surgical procedures with pain management standardized on surgery invasiveness and on expected level of postoperative pain; section P, randomized, included 41 women undergoing scheduled caesarean delivery with continuous intra-operative epidural anesthesia and post-operative analgesia (CEA). In both sections, POP was measured over 48 h (T6h-T24h-T48h) by the visual analogue scale (VAS). In section Pwe also tested the responsiveness of hypothalamic-pituitary-adrenal axis (HPA) expressed by cortisol levels. In section a , with cluster analysis, subjects were analyzed according to their genotype: a group (#1) of 34 patients reporting VAS score>3 at every time lapse was identified and included only A118G carriers, while wild-type (A118A -absence of 118A>G polymorphism) patients were unevenly distributed between those with cluster #2 (VAS score <3 at every study steps) and those with cluster #3 (VAS score progressively reducing from T6h). In section P, A118G carriers receiving epidural sufentanil had the lowest VAS scores at T24h; also in these patients, cortisol levels remained more stable, with a mild decrease at T6h. This study shows that theOPRMl 118A>G polymorphism affects postoperative pain response in heterozygous patients: they have a different postoperative pain response than patients with wild-type genes, which may affect the efficacy of the analgesic therapy.

show abstract

“…Так, Chou и соавт. показали, что при контролируемой пациентом аналгезии в раннем послеоперационном пе риоде после выполнения артропластики коленного сус тава носители генотипа 118G/G суммарно вводили себе большие дозы морфина (40,4±22 мг) по сравнению с но сительницами генотипа 118A/G (25,6±11,7 мг) и 118A/А (25,3±15,5 мг) [46]. В этом же исследовании по казано, что пациенты чаще вводили себе наркотический аналгетик по сравнению с носителями других геноти пов.…”

Section: Introductionunclassified

The Influence of Gene Polymorphism OPRM1 118A/G on the Perception of Pain and Pharmacodynamics of Narcotic Analgesics

Женило¹,

Махарин²

2014

rmt

View full text Add to dashboard Cite

Полиморфизм μ опиоидного рецептора является одним из наиболее изученных полиморфизмов, влияющих на актив ность наркотических аналгетиков. Несмотря на большое количество публикаций, посвященных данной проблеме, по лученные результаты в настоящее время не применяются в клинической практике. Целью данного обзора является описание влияний данного полиморфизма на восприятие болевого стимула и чувствительности к наркотическим ана лгетикам. Показано, что носители генотипа 118G/G μ опиоидного рецептора толерантны к действию наркотических аналгетиков и для достижения желаемого эффекта им требуется большая доза по сравнению с носителями нормаль ного генотипа. При этом вероятность возникновения побочных эффектов, связанных с назначением наркотических аналгетиков, существенно не отличается между носителями мажорного генотипа и носителями генотипов 118A/G, 118G/G. Ключевые слова: μ опиоидный рецептор, боль, фармакогенетика, аналгезия.

show abstract

Association of μ‐opioid receptor gene polymorphism (A118G) with variations in morphine consumption for analgesia after total knee arthroplasty

Cited by 283 publications

References 18 publications

Genetic variability of the μ-opioid receptor influences intrathecal fentanyl analgesia requirements in laboring women ☆

Genetic variability of the μ-opioid receptor influences intrathecal fentanyl analgesia requirements in laboring women ☆

Micro Opioid Receptor A118G Polymorphism and Post-Operative Pain: Opioids' Effects on Heterozigous Patients

The Influence of Gene Polymorphism OPRM1 118A/G on the Perception of Pain and Pharmacodynamics of Narcotic Analgesics

Contact Info

Product

Resources

About